Defective Transcription-Coupled Repair in Cockayne Syndrome B Mice Is Associated with Skin Cancer Predisposition

124

Cockayne Syndrome (CS) is a rare human genetic disorder characterized by progressive multisystem degeneration and segmental premature aging. The CS complementation group B (CSB) protein is engaged in transcription coupled and global nucleotide excision repair, base excision repair and general transcription. However, the precise molecular function of the CSB protein is still unclear. In the current review we discuss the involvement of CSB in some of these processes, with focus on the role of CSB in repair of oxidative damage, as deficiencies in the repair of these lesions may be an important aspect of the premature aging phenotype of CS.

Section: Clinical Manifestations Of Csmentioning

confidence: 99%

The role of Cockayne Syndrome group B (CSB) protein in base excision repair and aging

Stevnsner

Müftüoğlu

Aamann

et al. 2008

124

“…In humans, defects in the Cockayne syndrome (CS) A or B genes result in a transcriptional coupled NER defect, and these individuals exhibit growth failure, progressive neurological defects, along with kyphosis, osteoporosis, and a dramatically reduced mean life span of 12.5 years (Cleaver, 2005;Nance and Berry, 1992). Mice mutant for CS-B show some phenotypes of the human syndrome (van der Horst et al, 1997), but when crossed to NER-deficient Xpa-/-mice, the NER defect is complete and defective phenotypes are exacerbated, resembling those of the Ercc1-/-mice (van der Pluijm et al, 2007). The Csb m/m /Xpa-/-mice were growth retarded, exhibited multiple tissue defects, and had progeroid phenotypes, ultimately dying by 22 days of age.…”

Section: Suppression Of Igf-1 Signaling By Dna Damagementioning

confidence: 99%

How does suppression of IGF-1 signaling by DNA damage affect aging and longevity?

Hinkal

Donehower

2008

Long-lived animals have evolved a robust set of defenses to maintain genomic integrity over their entire lifespan. The DNA damage response and DNA repair pathways are critical pillars of organismal defenses, minimizing somatic mutations in both post-mitotic and mitotic cells. These genomic maintenance systems not only prevent the premature emergence of cancers, but may also maintain normal tissue function and organismal longevity. Genetic defects in a number of DNA repair and DNA damage response genes often leads to a dramatic increase in cancer incidence; in other cases, premature aging or progeroid syndromes may be induced. In this review, we discuss two recent reports of two nucleotide excision repair deficient models that exhibit dramatic premature aging and shortened longevity. The DNA repair defects were also associated with a significant inhibition of the growth hormone/insulin-like growth factor 1 (GH/IGF-1) axis, an endocrine signaling pathway shown to influence aging and longevity in both vertebrates and invertebrates. Potential mechanisms of how DNA damage might affect IGF-1 signaling and aging are discussed, with a particular emphasis on the role of such signaling alterations in the adult tissue stem cell compartments.

“…The neurodegenerative symptoms in mice are generally milder than in human and the cancer burden higher, especially for Cs (van der Horst et al, 1997;van der Horst et al, 2002;Laposa et al, 2007b) and Xpa De Vries, 1997;Tanaka et al, 2001). Variations due to strain backgrounds are also factors, especially regarding life-shortening versus cancer risk (Li et al, 2007;Partridge and Gems, 2007).…”

Section: What Constitutes Feasible Therapeutic Targets?mentioning

confidence: 99%

“…Variations due to strain backgrounds are also factors, especially regarding life-shortening versus cancer risk (Li et al, 2007;Partridge and Gems, 2007). The Cs-b strain that has been most extensively used (van der Horst et al, 1997;Laposa et al, 2007b) contains a truncation mutation that may resemble the mild human UV-sensitive disorder associated with an early truncation in CSB that lacks neurodegeneration (Horibata et al, 2004), unlike most CSB patients with amino acid changes and termination mutations scattered throughout the gene. There is consequently a need for further mouse models especially those that recapitulate the mutations causing severe CS clinical disorders.…”

Section: What Constitutes Feasible Therapeutic Targets?mentioning

confidence: 99%

Clinical implications of the basic defects in Cockayne syndrome and xeroderma pigmentosum and the DNA lesions responsible for cancer, neurodegeneration and aging

Cleaver

Revet

2008

Cancer, aging, and neurodegeneration are all associated with DNA damage and repair in complex fashions. Aging appears to be a cell and tissue-wide process linked to the insulin-dependent pathway in several DNA repair deficient disorders, especially in mice. Cancer and neurodegeneration appear to have complementary relationships to DNA damage and repair. Cancer arises from surviving cells, or even stem cells, that have down-regulated many pathways, including apoptosis, that regulate genomic stability in a multi-step process. Neurodegeneration however occurs in nondividing neurones in which the persistence of apoptosis in response to reactive oxygen species is, itself, pathological. Questions that remain open concern: sources and chemical nature of naturally occurring DNA damaging agents, especially whether mitochondria are the true source; the target tissues for DNA damage and repair; do the human DNA repair deficient diseases delineate specific pathways of DNA damage relevant to clinical outcomes; if naturally occurring reactive oxygen species are pathological in human repair deficient disease, would anti-oxidants or anti-apoptotic agents be feasible therapeutic agent?